A follow-up study of children born after intracytoplasmic sperm injection (ICSI) with epididymal and testicular spermatozoa and after replacement of cryopreserved embryos obtained after ICSI

doi:10.1093/humrep/13.suppl_1.196

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Human Reproduction, Vol. 13, No. suppl_1, pp. 196-207, 1998
© 1998 European Society of Human Reproduction and Embryology

A follow-up study of children born after intracytoplasmic sperm injection (ICSI) with epididymal and testicular spermatozoa and after replacement of cryopreserved embryos obtained after ICSI

M. Bonduelle¹^,3, A. Wilikens¹, A. Buysse¹, E. Van Assche¹, P. Devroey², A.C. Van Steirteghem² and I. Liebaers¹

¹ Centre for Medical Genetics, Medical Campus, Dutch-speaking Brussels Free University (Vrije Universiteit Brussel) Belgium ² Centre for Reproductive Medicine, Medical Campus, Dutch-speaking Brussels Free University (Vrije Universiteit Brussel) Belgium

Correspondence: ³To whom correspondence should be addressed at: Centre for Medical Genetics, Academisch Ziekenhuis V.U.B., Laarbeeklaan 101, 1090 Brussels, Belgium

The aim of this prospective follow-up study of children bornafter intracytoplasmic sperm injection (ICSI) was to compiledata on karyotypes, congenital malformations, growth parametersand developmental milestones in order to evaluate the safetyof this new technique. The study design included karyotypingof the parents and their agreement to genetic counselling andprenatal diagnosis and it was based on a physical examinationof the child at the Centre for Medical Genetics at the agesof 2 months, 1 year and at 2 years, where major and minor malformationsand psychomotor evolution are recorded. Here we describe thefirst 57 children born from 40 ICSI pregnancies with epididymalspermatozoa (group 1), the first 50 children born from 34 ICSIpregnancies with testicular spermatozoa (group 2) and the first58 children born from 48 pregnancies after replacement of cryopreservedICSI embryos (group 3). Parental karyotypes were obtained fromonly 72/246 (29%) parents and were all normal. Prenatal karyotypeswere determined for a total of 70 samples (40%): 21 in group1, 15 in group 2 and 34 in group 3. In this last group 2 abnormal47,XXY karyotypes (5.8%) and no structural aberrations werefound. This increase in denovo sex-chromosomal aberrations hasalready been described with regard to the first 877 childrenborn after ICSI carried out at our Centre and is probably linkeddirectly to the characteristics of the infertile men treatedrather than to the ICSI procedure itself. Major malformations,defined as those causing functional impairment or requiringsurgical correction, were observed in four children: two bornafter ICSI with epididymal spermatozoa, one after ICSI withtesticular spermatozoa and one after ICSI and cryopreservation.No particular malformation was disproportionally frequent. Inthe follow-up examinations at 2 months (107/161 or 66.5%) andat 1 year (37/161 or 22.9%), no additional anomalies were observed.Lost for follow-up rate at 2 months was 33.5%. These observationson a limited number of children do not suggest a higher incidenceof diseases linked to imprinting, nor do they suggest a higherincidence of congenital malformations. These observations arestill limited in number and should be further completed by othersand by collaborative efforts. In the meanwhile patients shouldbe told about the available data before any treatment: thereappears to be some risk of transmitted chromosomal aberrations,of de-novo, mainly sex-chromosomal aberrations and of transmittingfertility problems to the offspring. Patients should also bereassured that until now there seems to be no higher incidenceof congenital malformations in children born after ICSI withepididymal or testicular spermatozoa or after replacement ofICSI embryos.

Key words: children/congenital malformation/epididymal spermatozoa/intracytoplasmic sperm injection/pregnancy outcome/prenatal karyotypes/testicular spermatozoa

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